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在子宫内暴露于诺布啡,一种丁丙诺啡的主要代谢物,会导致胎儿阿片类药物依赖,并导致新生儿阿片类药物戒断综合征。

In Utero Exposure to Norbuprenorphine, a Major Metabolite of Buprenorphine, Induces Fetal Opioid Dependence and Leads to Neonatal Opioid Withdrawal Syndrome.

机构信息

Department of Chemistry and Biochemistry, University of Arkansas, Fayetteville, Arkansas (B.A.G.); Departments of Pharmacology and Toxicology (C.O.C., L.N.R., C.V.C., C.D.W., K.R.U., S.M.O., W.E.F., J.H.M., L.K.B.), Psychiatry (B.S.M.), and Microbiology and Immunology (M.D.Z.), University of Arkansas for Medical Sciences, Little Rock, Arkansas; and PinPoint Testing, LLC, Little Rock, Arkansas (A.L.P., A.W.A., J.H.M.).

Department of Chemistry and Biochemistry, University of Arkansas, Fayetteville, Arkansas (B.A.G.); Departments of Pharmacology and Toxicology (C.O.C., L.N.R., C.V.C., C.D.W., K.R.U., S.M.O., W.E.F., J.H.M., L.K.B.), Psychiatry (B.S.M.), and Microbiology and Immunology (M.D.Z.), University of Arkansas for Medical Sciences, Little Rock, Arkansas; and PinPoint Testing, LLC, Little Rock, Arkansas (A.L.P., A.W.A., J.H.M.)

出版信息

J Pharmacol Exp Ther. 2019 Jul;370(1):9-17. doi: 10.1124/jpet.118.254219. Epub 2019 Apr 26.

Abstract

Buprenorphine is the preferred treatment of opioid use disorder during pregnancy but can cause fetal opioid dependence and neonatal opioid withdrawal syndrome (NOWS). Notably, withdrawal severity is independent of maternal buprenorphine dose, suggesting that interindividual variance in pharmacokinetics may influence risk and severity of NOWS. Using a rat model of NOWS, we tested the hypothesis that clinically relevant doses of the active metabolite norbuprenorphine (NorBUP) can induce in utero opioid dependence, manifested as naltrexone-precipitated withdrawal signs in the neonate. Pregnant Long-Evans rats were implanted with 14-day osmotic minipumps containing vehicle, morphine (positive control), or NorBUP (0.3-10 mg/kg per day) on gestation day 9. By 12 hours post-delivery, an intraperitoneal injection of the opioid antagonist naltrexone (1 or 10 mg/kg) or saline was administered to pups. Precipitated withdrawal signs were graded by raters blinded to treatment conditions. In a separate group, NorBUP concentrations in maternal and fetal blood and brain on gestation day 20 were determined by liquid chromatography-tandem mass spectrometry. Steady-state maternal blood concentrations of NorBUP in dams infused with 1 or 3 mg/kg per day were comparable to values reported in pregnant humans treated with buprenorphine (1.0 and 9.6 ng/ml, respectively), suggesting a clinically relevant dosing regimen. At these doses, NorBUP increased withdrawal severity in the neonate as shown by an evaluation of 10 withdrawal indicators. These findings support the possibility that NorBUP contributes to fetal opioid dependence and NOWS following maternal buprenorphine treatment during pregnancy.

摘要

丁丙诺啡是治疗妊娠期间阿片类药物使用障碍的首选药物,但会导致胎儿阿片类药物依赖和新生儿阿片类戒断综合征(NOWS)。值得注意的是,戒断严重程度与母体丁丙诺啡剂量无关,这表明个体间药代动力学的差异可能会影响 NOWS 的风险和严重程度。我们使用大鼠 NOWS 模型来检验以下假设,即临床相关剂量的活性代谢物诺丁丙诺啡(NorBUP)可诱导胎儿阿片类药物依赖,表现为新生儿纳曲酮诱发的戒断症状。在妊娠第 9 天,将含有载体、吗啡(阳性对照)或 NorBUP(0.3-10mg/kg/天)的 14 天渗透微型泵植入孕鼠体内。分娩后 12 小时,对幼鼠进行腹腔内注射阿片拮抗剂纳曲酮(1 或 10mg/kg)或生理盐水。由对治疗条件不知情的评估者对诱发的戒断症状进行分级。在另一组中,通过液相色谱-串联质谱法测定妊娠第 20 天母鼠和胎儿血液及脑组织中的 NorBUP 浓度。每天输注 1 或 3mg/kg 的 NorBUP 时,母体血液中的 NorBUP 稳态浓度与接受丁丙诺啡治疗的孕妇(分别为 1.0 和 9.6ng/ml)中的报告值相当,提示存在临床相关的给药方案。在这些剂量下,NorBUP 增加了新生儿的戒断严重程度,这可以通过对 10 个戒断指标的评估来证明。这些发现支持了这样一种可能性,即 NorBUP 可能会导致母体在妊娠期间接受丁丙诺啡治疗后胎儿阿片类药物依赖和 NOWS。

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